SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2897923283> ?p ?o ?g. }

Showing items 1 to 81 of 81 with 100 items per page.

W2897923283 abstract "Glioblastoma multiforme is a highly invasive and incurable primary brain tumor. The most frequent genetic alteration therein is amplification of the epidermal growth factor receptor (EGFR) gene, the target of current clinical trials. However, EGFR amplification is poorly represented in glioblastoma cell lines. From the 30 cultures attempted herein, we were able to establish two glioblastoma permanent cell lines. The remaining cultures showed limited life span and underwent senescence between passage numbers (PN) 8 to 15. Our newly established glioblastoma cell lines, designated 170-MG-BA and 538-MG-BA, both originated between PN 3 and 5 when areas of smaller, more rapidly proliferating cells appeared. Both cell lines showed similar rates of growth, moderate morphological differences, cytoskeletal heterogeneity and multiple chromosome rearrangements. Analysis by molecular cytogenetics and comparative genomic hybridization (aCGH) revealed two copies of a stable marker chromosome in 170-MG-BA cells effecting focal amplification at 7q11 of the EGFR locus. Comparative RqPCR analysis confirmed that EGFR was uniquely highly expressed in 170-MG-BA cells. Combined targeted expression analysis and aCGH data excluded the recurrent EGFRvIII activating mutation. In contrast, EGFR expression in 538-MG-BA cells which lacked genomic EGFR amplification was not raised. Immunofluorescent staining showed high EGFR protein expression only in the 170-MG-BA cells. Cytogenetic, genomic and transcriptional analyses then confirmed high-level genomic amplification and transcriptional upregulation of wild type EGFR in 170-MG-BA; the first conventional cell line model for investigating the biology and targeted therapy of this key alteration in glioblastoma. Both cell lines are freely available from the DSMZ cell repository." @default.
W2897923283 created "2018-10-26" @default.
W2897923283 creator A5010000664 @default.
W2897923283 creator A5014792699 @default.
W2897923283 creator A5016264990 @default.
W2897923283 creator A5028192601 @default.
W2897923283 creator A5064242864 @default.
W2897923283 creator A5071081889 @default.
W2897923283 creator A5077399010 @default.
W2897923283 creator A5088371729 @default.
W2897923283 date "2019-01-01" @default.
W2897923283 modified "2023-09-28" @default.
W2897923283 title "High level EGFR amplification in a newly established glioblastoma cell line 170-MG-BA" @default.
W2897923283 doi "https://doi.org/10.4149/neo_2018_180427n278" @default.
W2897923283 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30509096" @default.
W2897923283 hasPublicationYear "2019" @default.
W2897923283 type Work @default.
W2897923283 sameAs 2897923283 @default.
W2897923283 citedByCount "2" @default.
W2897923283 countsByYear W28979232832019 @default.
W2897923283 countsByYear W28979232832021 @default.
W2897923283 crossrefType "journal-article" @default.
W2897923283 hasAuthorship W2897923283A5010000664 @default.
W2897923283 hasAuthorship W2897923283A5014792699 @default.
W2897923283 hasAuthorship W2897923283A5016264990 @default.
W2897923283 hasAuthorship W2897923283A5028192601 @default.
W2897923283 hasAuthorship W2897923283A5064242864 @default.
W2897923283 hasAuthorship W2897923283A5071081889 @default.
W2897923283 hasAuthorship W2897923283A5077399010 @default.
W2897923283 hasAuthorship W2897923283A5088371729 @default.
W2897923283 hasBestOaLocation W28979232831 @default.
W2897923283 hasConcept C104317684 @default.
W2897923283 hasConcept C120821319 @default.
W2897923283 hasConcept C124942203 @default.
W2897923283 hasConcept C141231307 @default.
W2897923283 hasConcept C150194340 @default.
W2897923283 hasConcept C153911025 @default.
W2897923283 hasConcept C170493617 @default.
W2897923283 hasConcept C2779438470 @default.
W2897923283 hasConcept C30481170 @default.
W2897923283 hasConcept C502942594 @default.
W2897923283 hasConcept C54355233 @default.
W2897923283 hasConcept C55548728 @default.
W2897923283 hasConcept C7602840 @default.
W2897923283 hasConcept C81885089 @default.
W2897923283 hasConcept C84597430 @default.
W2897923283 hasConcept C86803240 @default.
W2897923283 hasConceptScore W2897923283C104317684 @default.
W2897923283 hasConceptScore W2897923283C120821319 @default.
W2897923283 hasConceptScore W2897923283C124942203 @default.
W2897923283 hasConceptScore W2897923283C141231307 @default.
W2897923283 hasConceptScore W2897923283C150194340 @default.
W2897923283 hasConceptScore W2897923283C153911025 @default.
W2897923283 hasConceptScore W2897923283C170493617 @default.
W2897923283 hasConceptScore W2897923283C2779438470 @default.
W2897923283 hasConceptScore W2897923283C30481170 @default.
W2897923283 hasConceptScore W2897923283C502942594 @default.
W2897923283 hasConceptScore W2897923283C54355233 @default.
W2897923283 hasConceptScore W2897923283C55548728 @default.
W2897923283 hasConceptScore W2897923283C7602840 @default.
W2897923283 hasConceptScore W2897923283C81885089 @default.
W2897923283 hasConceptScore W2897923283C84597430 @default.
W2897923283 hasConceptScore W2897923283C86803240 @default.
W2897923283 hasLocation W28979232831 @default.
W2897923283 hasLocation W28979232832 @default.
W2897923283 hasOpenAccess W2897923283 @default.
W2897923283 hasPrimaryLocation W28979232831 @default.
W2897923283 hasRelatedWork W1992478949 @default.
W2897923283 hasRelatedWork W1996760590 @default.
W2897923283 hasRelatedWork W2028976524 @default.
W2897923283 hasRelatedWork W2045072898 @default.
W2897923283 hasRelatedWork W2047042799 @default.
W2897923283 hasRelatedWork W2067963031 @default.
W2897923283 hasRelatedWork W2155557383 @default.
W2897923283 hasRelatedWork W2609105076 @default.
W2897923283 hasRelatedWork W2738096720 @default.
W2897923283 hasRelatedWork W2950943363 @default.
W2897923283 isParatext "false" @default.
W2897923283 isRetracted "false" @default.
W2897923283 magId "2897923283" @default.
W2897923283 workType "article" @default.